DE4318577A1 - Lubricant-free, medicament-containing tablets - Google Patents

Abstract

The invention relates to lubricant-free tablets which contain a pharmaceutical agent and are based on microcrystalline cellulose with a content of at least 85% in comparison with the complete tablet composition. The invention relates in particular to corresponding tablets which contain as pharmaceutical agent hormones, preferably thyroid hormones.

Description

The invention relates to new lubricant-free tablets based on microcri stalliner cellulose, which contain an active pharmaceutical ingredient as well as if necessary, agents that improve the wettability and disintegration of the tablet mass heights. The tablets of the invention consist of at least 85% (w / w) microcrystalline cellulose. In particular, the invention relates to corresponding Tablets used as an active pharmaceutical ingredient hormones, preferably shield contain gland hormones or agents that affect the thyroid gland.

When tableting pharmaceutical mixtures are usually Lubricant used so that the press tools are constantly lubricated and good mold separation is guaranteed. They also effect training a smooth tablet surface. Common physiolo suitable for this purpose gisch compatible lubricants are, for example, magnesium stearate or Mixtures of silicone oil with highly disperse silicon dioxide. Such lubrication Medium also have disadvantages. So they cause most mixes are more difficult to compress. You have to have relatively high press forces (over 10 kN) to obtain useful tablets. This in turn brings naturally a faster wear of the tabletting tools. Wei furthermore, the known lubricants have the disadvantage that they are often quick counteract and complete release of the active pharmaceutical ingredient. This is particularly important when the are used Active ingredients in relation to the total tablet mass only in small doses (<5%) can be.

The task was therefore to provide medicinal tablets to be able to overcome the known disadvantages with regard to the effect of the lubricant not have.

It has now been found that lubricants can be dispensed with entirely, if microcrystalline cellulose is used as the carrier. The weight percentage According to the invention, the microcrystalline cellulose must be at least 85%.  

The invention thus relates to a lubricant-free medicinal product Tablet based on microcrystalline cellulose with a content of at least 85% (w / w). It is preferably between 90 and 98%, in particular between 93 and 96% (w / w).

According to the invention, commercially available purified microcrystalline cellulose is used a grain size of 50 to 400, preferably 150 to 250 microns as a carrier, the replaced the usual tablet carriers such as mannitol or lactose.

The invention also relates to corresponding tablets which contain a hydro contain philorizing agents, the content preferably being at most 5%, especially 1 to 3%.

According to the invention, such auxiliaries are referred to as hydrophilizing agents net, which increase the wetting of the tablet mass. Appropriate hydrophilicity All water-soluble cellulose derivatives, such as, for example, hydroxyl, are used propyl cellulose or hydroxyethyl cellulose, sugar, such as. B. sucrose or Lactose, sugar alcohols such as B. sorbitol or mannitol but also polyvinylpyrroli don, polyethylene glycols or surfactants, such as. B. sodium lauryl sulfate.

The invention also relates to a corresponding tablet, which is a decay contains the tablet-promoting agent (disintegrant), preferably with a Content of maximum 5%, in particular 1 to 3.5% compared to the total Tablet mass.

Crosslinked cellulose derivatives such as, for example, are suitable as disintegrants Sodium carboxymethyl cellulose, cross-linked polyvinyl pyrrolidone, sodium starch glycolate or modified starches.

The tablets according to the invention preferably contain both hydrophilicity as well as explosives. Depending on the dosage and solubility of the used Active pharmaceutical ingredient can hydrophilizing agents or both Aids are left out.  

The invention particularly relates to a corresponding tablet, which as Active ingredient is a thyroid hormone (thyroxine) or one that affects the thyroid Contains agents such as potassium iodide.

However, other pharmaceutical formulations are also available for the new tablet formulations Active substances are suitable, especially those that can only be dosed in small quantities special attention must be paid to their stability. In addition, are particularly suitable the thyroxines mentioned Adrenal hormones and analogous substances (corticoids such as Dexa methasone, deoxymethasone or halomethasone), hormones such as sex hormones (e.g. ethinyl estradiol, chloromadinone acetate), anabolic steroids or parathyroid glands hormones. The proportion of the active ingredient concentration in the total tablet mass should Do not exceed 5% (w / w), otherwise the rapid and complete release of the Active ingredient can be adversely affected. Tablets are preferred prepared, the proportion of which is 0.05 to 3%, in particular 0.1 to 1%.

The new tablet formulations result in an almost quantitative rapid release setting of active ingredients, especially thyroid hormones. So z. B. 95 to 100% of thyroxines within 60 minutes from the invention Lubricant-free tablet mass released. In contrast, Thy roxine at the same dosage (approx. 0.1%) from tablet masses based on Mannitol in the presence of a lubricant required for this (e.g. silicone oil / SiO₂) only about 30 to 50% released in the same time. This after the State of the art bad release of thyroxine is also caused by very low requirements taken into account in official monographs (USP XXII: "Levothyroxine Sodium Tablets": 55% within 80 minutes). The verbes Serte release rates are also with the other drugs mentioned achieve. This can be described as surprising, since microcrystalline Cellulose is sparingly soluble, and losses due to adsorption effects are not general can be excluded.  

For stability-sensitive drugs such as B. the thyroxines is usually in tablet formulations of the prior art (with lubricant) one for Considerable initial decomposition rate (during the manufacturing process) observed, which until now could only be countered by production surcharges. So losses of z. B. Levothyroxine from 5 to 15%, whichever Carrier and which lubricant is used. In the case of the invention Tablet formulation, however, are only losses through decomposition up to a maximum 1% observed. Production surcharges can therefore be omitted. Also with regard Lich the storage stability of the tablets according to the invention have improved properties create. After 6 months there are only between 1 and 3% losses in the Compared to more than 5% loss in lubricant-containing tablet form observations.

By omitting the lubricant in the tablets according to the invention Manufacturing usually simplifies and makes the manufacturing process cheaper by saving one operation. In addition, there are only small pressing forces required to obtain high quality tablets (3 to 6 kN in ver equal to 12 to 16 kN in the presence of a lubricant using of carriers of the prior art). The low pressing forces allow careful handling and therefore a longer shelf life of the tabletting unit witness.

The invention thus ultimately relates to a method for producing lubricant-free, drug-containing tablets, which is characterized by that microcrystalline cellulose with the active ingredient in powder or dissolved form if desired, mixed together with auxiliaries and, if necessary, after drying pressed directly into tablets, the content of microcrystalline cellulose is at least 85% (w / w) and the required pressing forces preferably between between 3 and 6 kN.

With the aid of the method according to the invention, significantly more tablets can also be used ten per unit of time. So the tableting speed is about 2 to 3 times higher than with the conventional methods mentioned. Especially the method according to the invention works effectively when the pharmaceutical  Active ingredient in dissolved form, preferably in methanolic solution of the tablets mass is added. In addition to methanol and ethanol, ketonic ones are also suitable Solvents (e.g. acetone) or mixtures of the solvents mentioned, if the solubility of the drug in it is sufficient.

The following examples are intended to explain the invention further.

example 1

141.4 kg microcrystalline cellulose (180 to 200 µm), 3 kg hydroxypropyl methyl cellulose and 5.3 kg carboxymethyl cellulose sodium (cross-linked) placed in a high speed mixer and intense for about 20 minutes mixed. 0.18 kg of levothyroxine sodium and 0.2 kg of potassium iodide are dissolved in 20 liters of methanol and mix the mass with the methanolic solution. The The tablet mass is then in the high-speed mixer at a maximum of 28 dried to 30 ° C for about 90 minutes and then by means of a commercial usual tableting machine with a pressing force of 3 to 4 kN for a tableting speed of 200,000 to 300,000 tablets / h pressed into tablets. Man receives approximately 1,500,000 tablets with a drug content of approximately 0.12%.

Example 2

Tablets containing thyroxine are produced analogously to Example 1. Instead of Hydroxypropycellulose uses the same amount of polyvinylpyrrolidone as Hydrophi lizing agent used.

Example 3

Tablets containing thyroxine are produced analogously to Example 1. Instead of Cross-linked carboxymethyl cellulose is called the same amount of sodium glycolate Explosives used.  

Example 4

Analogously to Example 1, tablets are produced which contain 0.3% levthyroxine sodium but does not contain potassium iodide.

Example 5

Analogously to Example 1, tablets are produced which contain only potassium iodide as the active ingredient (0.1%) included.

Example 6

Microcrystalline cellulose, sodium starch glycolate and Fludrocortisone dry mixed together and in a given way Tablets pressed. The active substance content of the tablets is 0.2%.

Example 7

Analogously to Example 5, tablets are produced which contain dexamethasone as the active ingredient (1%) included.

Example 8

Analogously to example 6, tablets are produced which contain prednisolone (3%) as active ingredient. contain.

Example 9

Analogously to Example 1, tablets are produced which contain ethinylestradiol as the active ingredient (0.05%) included.  

Example 10 (comparative example, prior art)

127.5 kg of mannitol are placed in the high-speed mixer. Potassium iodide (0.2 kg) and levothyroxine sodium (0.18 kg) are dissolved in 20 liters of methanol and abandoned with stirring. Then at about 26 to 28 ° C for about 90 minutes dried long. This is followed by the introduction of 1.5 kg of highly disperse silicon dioxide, 17.6 kg of microcrystalline cellulose (approx. 10%) and 3 kg of a 50% mixture of highly disperse silicon dioxide in silicone oil (Silicon-Aerosil®, lubricant). The mass is mixed intensively for about 20 minutes. After a salary determination Levothyroxine sodium becomes a methanoli according to the loss mixed solution of levothyroxine sodium and dried. The mass is finally at 14 to 16 kN and the maximum under these conditions possible tablet speed of 100,000 tablets / h pressed into tablets. About 1,500,000 tablets with a drug content of about 0.12% are obtained.

Example 11 (drug release)

A defined amount of tablets produced according to Example 1 or Example 5 are tested in the release apparatus according to the German Pharmacopoeia and according to 80 minutes of the dissolved drug content according to known methods certainly. The same procedure is followed with tablets manufactured according to Example 10 were.

Example 12 (stability)

The content of active ingredient in the finished compressed tablet is immediately after tableting process (initial stability) and after six months (storage stability) determined by known methods. Get the values after 6 months the initial values determined after tableting was completed (adjusted for initial decomposition).

Claims (14)

1. Lubricant-free, drug-containing tablet based on microcrystalline Cellulose with a content of at least 85% (w / w). 2. Tablet according to claim 1, characterized in that it is a hydrophilic contains agent. 3. Tablet according to claim 2, characterized in that the content of hydro Philization funds is a maximum of 5% (w / w). 4. Tablet according to claim 2 or 3, characterized in that the hydrophi lizing agent is a water-soluble cellulose derivative. 5. Tablet according to one of claims 1 to 4, characterized in that it contains a disintegrant that promotes the disintegration of the tablet. 6. Tablet according to claim 5, characterized in that the content of Disintegrant is a maximum of 5% (w / w). 7. Tablet according to claim 5 or 6, characterized in that the blasting medium is a cross-linked cellulose derivative. 8. Tablet according to one of claims 1 to 7, characterized in that the Active pharmaceutical ingredient is a maximum of 5% (w / w). 9. Tablet according to claim 8, characterized in that the active ingredient Is thyroid hormone or an agent that affects the thyroid gland. 10. Process for the production of lubricant-free medicinal products Tablets, characterized in that microcrystalline cellulose with the active ingredient in powder or dissolved form if desired together with Auxiliaries mixed and, if necessary, pressed directly into tablets after drying, the microcrystalline cellulose content being at least 85% (w / w).   11. The method according to claim 10, characterized in that as an aid Hydrophilizing agent and / or one which promotes the disintegration of the tablet By means of (disintegrant) is added. 12. The method according to claim 10 or 11, characterized in that the Mix components are pressed with a pressure of 3 to 6 kN. 13. The method according to any one of claims 10 to 12, characterized in that a thyroid hormone is used as an active ingredient. 14. The method according to claim 13, characterized in that the active ingredient in methanolic solution is introduced into the mixture.